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RORγt-driven TH17 Cell Differentiation Requires Epigenetic Control by the Swi/Snf Chromatin Remodeling Complex

Sungkyu Lee, Ji‐Eun Kim, Hyungyu Min, Rho Hyun Seong

2020iScience24 citationsDOIOpen Access PDF

Abstract

Epigenetic regulation, including chromatin accessibility and posttranslational modifications of histones, is of importance for T cell lineage decision. TH17 cells play a critical role in protective mucosal immunity and pathogenic multiple autoimmune diseases. The differentiation of TH17 cells is dictated by a master transcription factor, RORγt. However, the epigenetic mechanism that controls TH17 cell differentiation remains poorly understood. Here we show that the Swi/Snf complex is required for TH17-mediated cytokine production both in vitro and in vivo. We demonstrate that RORγt recruits and forms a complex with the Swi/Snf complex to cooperate for the RORγt-mediated epigenetic modifications of target genes, including both permissive and repressive ones for TH17 cell differentiation. Our findings thus highlight the Swi/Snf complex as an essential epigenetic regulator of TH17 cell differentiation and provide a basis for the understanding of how a master transcription factor RORγt collaborates with the Swi/Snf complex to govern epigenetic regulation.

Topics & Concepts

EpigeneticsSWI/SNFChromatin remodelingTranscription factorChromatinBiologyRAR-related orphan receptor gammaCell biologyCellular differentiationHistoneGeneticsGeneIL-33, ST2, and ILC PathwaysT-cell and B-cell ImmunologyImmune Cell Function and Interaction